Differential Inhibition by Selective Phosphodiesterase Inhibitors of Antigen, LTC4and Histamine-induced Contraction of Guinea-pig Isolated Trachea

Pulmonary pharmacology Pub Date : 1996-08-01 DOI:10.1006/pulp.1996.0032

J.-M. Planquois , Y. Ruffin-Morin , V. Lagente , A.N. Payne , S.G. Dahl

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引用次数: 3

Abstract

Antigen (ovalbumin)-induced contraction of guinea-pig isolated trachea, which largely resulted from the endogenous release of peptidoleukotrienes, was strongly inhibited by the non-selective phosphodiesterase (PDE) inhibitor theophylline and, more potently, by the selective PDE type IV inhibitors rolipram and Ro 20-1724. It was also strongly inhibited by the PDE type V inhibitor zaprinast, but much less so by the PDE type III inhibitor siguazodan and milrinone. Similar results were obtained in trachea minus epithelium. In contrast to their effects vs. allergic airway smooth muscle contraction, both milrinone and siguazodan potently relaxed leukotriene C₄(LTC₄)-induced contraction in isolated trachea from non-sensitized animals. In this assay, rolipram, Ro 20-1724 and zaprinast were less active compared to their effects vs. ovalbumin-induced contraction, whereas theophylline had equivalent potency in the two tests. The relative potencies of rolipram and siguazodan in relaxation of trachea were similar when added prior to or after either LTC₄or histamine. These results suggest that the higher potency of selective PDE type IV & V inhibitors compared with PDE type III inhibitors vs. ovalbumin-induced contraction is due to their greater inhibition of anaphylactic mediator release. The converse is true if we consider their bronchodilator actions, although the superior efficacy of selective PDE type III inhibitors over PDE type IV inhibitors may vary in sensitized vs. non-sensitized animals. The present results are in agreement with a previous study showing that low concentrations of aβ₂-agonist increased the relaxant effect of selective PDE type IV inhibitors in guinea-pig trachea. The present data indicate that prophylactic use of selective PDE type IV inhibitors combined with therapeutic use of low dose inhaledβ-agonists might represent an alternative to the use of anti-allergic or steroid therapy in asthma.

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选择性磷酸二酯酶抑制剂抗原、ltc4和组胺诱导豚鼠离体气管收缩的差异抑制作用

抗原(卵清蛋白)诱导的豚鼠离体气管收缩主要由内源性肽多溴三烯释放引起，非选择性磷酸二酯酶(PDE)抑制剂茶碱和选择性磷酸二酯酶IV型抑制剂罗利普兰和ro20 -1724对其有较强的抑制作用。PDE V型抑制剂zaprinast对其也有强烈的抑制作用，但PDE III型抑制剂siguazodan和milrinone对其的抑制作用要小得多。在气管无上皮细胞中也得到了类似的结果。与它们对过敏性气道平滑肌收缩的作用相反，米力酮和西格唑丹都能有效地放松白三烯C4(LTC4)诱导的非致敏动物离体气管收缩。在这个实验中，罗利普兰，ro20 -1724和zaprinast的活性低于它们对卵清蛋白诱导的收缩的作用，而茶碱在两个测试中具有相同的效力。氟利普兰和西氟唑丹在ltc4或组胺之前或之后使用时，对气管舒张作用的相对效力相似。这些结果表明选择性PDE IV型和amp;与PDE III型抑制剂相比，V型抑制剂与卵清蛋白诱导的收缩是由于它们对过敏介质释放的抑制更大。如果我们考虑它们的支气管扩张作用，则相反，尽管在致敏动物和非致敏动物中，选择性PDE III型抑制剂优于PDE IV型抑制剂的疗效可能有所不同。目前的结果与先前的研究一致，表明低浓度的a- β2激动剂增加了选择性PDE IV型抑制剂在豚鼠气管中的松弛作用。目前的数据表明，预防性使用选择性PDE IV型抑制剂联合治疗性使用低剂量吸入β激动剂可能是哮喘抗过敏或类固醇治疗的替代方法。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Pulmonary pharmacology

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